血清素转运体基因变异与饲养条件对雌性灵长类动物酒精偏好和摄入量的相互作用。
Interaction between serotonin transporter gene variation and rearing condition in alcohol preference and consumption in female primates.
作者信息
Barr Christina S, Newman Timothy K, Lindell Stephen, Shannon Courtney, Champoux Maribeth, Lesch Klaus Peter, Suomi Stephen J, Goldman David, Higley J Dee
机构信息
National Institute on Alcoholism and Alcohol Abuse, Laboratory of Clinical Studies and National Institute of Child Health and Human Development, Laboratory of Comparative Ethology, National Institutes of Health, Poolesville, MD, USA.
出版信息
Arch Gen Psychiatry. 2004 Nov;61(11):1146-52. doi: 10.1001/archpsyc.61.11.1146.
BACKGROUND
Serotonin neurotransmission and limbic-hypothalamic-pituitary-adrenal (LHPA) axis hormones are thought to be involved in the reinforcement of alcohol intake and contribute to the risk for alcoholism. In humans and macaques, a promoter polymorphism that decreases transcription of the serotonin transporter gene is associated with anxiety and altered LHPA-axis responses to stress, and in female macaques, exposure to early-life stress alters LHPA-axis activation in response to alcohol. We wanted to determine whether serotonin transporter gene promoter variation (rh-5HTTLPR) and rearing condition would interact to influence alcohol preference in female rhesus macaques. Because of the involvement of stress and LHPA-axis activity in symptoms of withdrawal and relapse, we also wanted to determine whether serotonin transporter gene variation and rearing condition would influence changes in the patterns of alcohol consumption across a 6-week alcohol consumption paradigm.
METHODS
Female macaques were reared with their mothers in social groups (n = 18) or in peer-only groups (n = 14). As young adults, they were given access to an aspartame-sweetened 8.4% alcohol solution and vehicle for 1 hour per day, and volumes of consumption of alcoholic and nonalcoholic solutions were recorded. Serotonin transporter genotype (l/l and l/s) was determined using polymerase chain reaction followed by gel electrophoresis.
RESULTS
We found interactions between rearing condition and serotonin transporter genotype, such that l/s peer-reared females demonstrated higher levels of ethanol preference. We also found an effect of rearing condition on the percentage change in alcohol consumed during the 6 weeks as well as a phase by rearing interaction, such that peer-reared animals progressively increased their levels of consumption across the course of the study. This was especially evident for peer-reared females with the l/s rh5-HTTLPR genotype.
CONCLUSION
These data suggest a potential interaction between serotonin transporter gene variation and early experience in vulnerability to alcoholism.
背景
血清素神经传递和边缘-下丘脑-垂体-肾上腺(LHPA)轴激素被认为参与了酒精摄入的强化过程,并导致酒精成瘾风险。在人类和猕猴中,一种降低血清素转运体基因转录的启动子多态性与焦虑以及LHPA轴对应激的反应改变有关,并且在雌性猕猴中,早年应激暴露会改变LHPA轴对酒精的激活反应。我们想要确定血清素转运体基因启动子变异(rh-5HTTLPR)和饲养条件是否会相互作用,影响雌性恒河猴的酒精偏好。由于应激和LHPA轴活动参与了戒断和复发症状,我们还想要确定血清素转运体基因变异和饲养条件是否会影响在为期6周的酒精消费范式中酒精消费模式的变化。
方法
雌性猕猴在社会群体中与母亲一起饲养(n = 18)或仅与同伴一起饲养(n = 14)。成年后,每天给它们提供1小时的阿斯巴甜加甜的8.4%酒精溶液和对照溶液,并记录酒精和非酒精溶液的消费量。使用聚合酶链反应随后进行凝胶电泳来确定血清素转运体基因型(l/l和l/s)。
结果
我们发现饲养条件和血清素转运体基因型之间存在相互作用,使得同伴饲养的l/s雌性猕猴表现出更高的乙醇偏好水平。我们还发现饲养条件对6周内酒精消费的百分比变化有影响,以及饲养条件与阶段之间的相互作用,使得同伴饲养的动物在研究过程中逐渐增加其消费水平。这在具有l/s rh5-HTTLPR基因型的同伴饲养雌性猕猴中尤为明显。
结论
这些数据表明血清素转运体基因变异与早年经历在酒精成瘾易感性方面可能存在相互作用。
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